Macrophage interactions with neutrophils regulate Leishmania major infection

被引：177

作者：

Ribeiro-Gomes, FL

Otero, AC

Gomes, NA

Moniz-De-Souza, MCA

Cysne-Finkelstein, L

Arnholdt, AC

Calich, VL

Coutinho, SG

Lopes, MF

DosReis, GA

机构：

[1] Fed Univ Rio De Janeiro, Inst Biofis Carlos Chagas Filho, Programa Imunobiol, BR-21949900 Rio De Janeiro, Brazil

[2] Fundacao Oswaldo Cruz, Inst Oswaldo Cruz, Rio De Janeiro, Brazil

[3] Univ Sao Paulo, Inst Ciencias Biomed, BR-05508 Sao Paulo, Brazil

来源：

JOURNAL OF IMMUNOLOGY | 2004年 / 172卷 / 07期

关键词：

D O I：

10.4049/jimmunol.172.7.4454

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Macrophages are host cells for the pathogenic parasite Leishmania major. Neutrophils die and are ingested by macrophages in the tissues. We investigated the role of macrophage interactions with inflammatory neutrophils in control of L. major infection. Coculture of dead exudate neutrophils exacerbated parasite growth in infected macrophages from susceptible BALB, but killed intracellular L. major in resistant B6 mice. Coinjection of dead neutrophils amplified L. major replication in vivo in BALB, but prevented parasite growth in 136 mice. Neutrophil depletion reduced parasite load in infected BALB, but exacerbated infection in B6 mice. Exacerbated growth of L. major required PGE(2) and TGF-beta production by macrophages, while parasite killing depended on neutrophil elastase and TNF-alpha production. These results indicate that macrophage interactions with dead nentrophils play a previously unrecognized role in host responses to L. major infection.

引用

页码：4454 / 4462

页数：9

共 52 条

[1] Dipeptidyl peptidase I activates neutrophil-derived serine proteases and regulates the development of acute experimental arthritis [J].

Adkison, AM ;

Raptis, SZ ;

Kelley, DG ;

Pham, CTN .

JOURNAL OF CLINICAL INVESTIGATION, 2002, 109 (03) :363-371

[2] TRANSFORMING GROWTH-FACTOR-BETA IN LEISHMANIAL INFECTION - A PARASITE ESCAPE MECHANISM [J].

BARRALNETTO, M ;

BARRAL, A ;

BROWNELL, CE ;

SKEIKY, YAW ;

ELLINGSWORTH, LR ;

TWARDZIK, DR ;

REED, SG .

SCIENCE, 1992, 257 (5069) :545-548

[3] DIFFERENCES IN THE ONSET OF THE INFLAMMATORY RESPONSE TO CUTANEOUS LEISHMANIASIS IN RESISTANT AND SUSCEPTIBLE MICE [J].

BEIL, WJ ;

MEINARDUSHAGER, G ;

NEUGEBAUER, DC ;

SORG, C .

JOURNAL OF LEUKOCYTE BIOLOGY, 1992, 52 (02) :135-142

[4] Organ-specific and stage-dependent control of Leishmania major infection by inducible nitric oxide synthase and phagocyte NADPH oxidase [J].

Blos, M ;

Schleicher, U ;

Rocha, FJS ;

Meissner, U ;

Röllinghoff, M ;

Bogdan, C .

EUROPEAN JOURNAL OF IMMUNOLOGY, 2003, 33 (05) :1224-1234

[5] Invasion, control and persistence of Leishmania parasites [J].

Bogdan, C ;

Gessner, A ;

Solbach, W ;

Rollinghoff, M .

CURRENT OPINION IN IMMUNOLOGY, 1996, 8 (04) :517-525

[6] MACROPHAGE ENGULFMENT OF APOPTOTIC NEUTROPHILS CONTRIBUTES TO THE RESOLUTION OF ACUTE PULMONARY INFLAMMATION IN-VIVO [J].

COX, G ;

CROSSLEY, J ;

XING, Z .

AMERICAN JOURNAL OF RESPIRATORY CELL AND MOLECULAR BIOLOGY, 1995, 12 (02) :232-237

[7] Macrophages that have ingested apoptotic cells in vitro inhibit proinflammatory cytokine production through autocrine/paracrine mechanisms involving TGF-β, PGE2, and PAF [J].

Fadok, VA ;

Bratton, DL ;

Konowal, A ;

Freed, PW ;

Westcott, JY ;

Henson, PM .

JOURNAL OF CLINICAL INVESTIGATION, 1998, 101 (04) :890-898

[8] Differential effects of apoptotic versus lysed cells on macrophage production of cytokines: Role of proteases [J].

Fadok, VA ;

Bratton, DL ;

Guthrie, L ;

Henson, PM .

JOURNAL OF IMMUNOLOGY, 2001, 166 (11) :6847-6854

[9]

FARRELL JP, 1987, J IMMUNOL, V138, P902

[10] p38 mitogen-activated protein kinase-dependent and -independent intracellular signal transduction pathways leading to apoptosis in human neutrophils [J].

Frasch, SC ;

Nick, JA ;

Fadok, VA ;

Bratton, DL ;

Worthen, GS ;

Henson, PM .

JOURNAL OF BIOLOGICAL CHEMISTRY, 1998, 273 (14) :8389-8397

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